Complete resolution of the side effect with efficacy has been reported in 72% and 86% of patients treated in this way.[49, 53] Thiopurine-induced pancreatitis occurs in approximately 4% of patients[38] MAPK Inhibitor Library supplier and has been considered a strict contraindication to subsequent treatment with an alternative thiopurine.[75] Three small retrospective case series (< 10 patients each) have examined rechallenging patients with 6MP after AZA-induced pancreatitis, with overall success rates varying from 29% to 100%.[76-78] There are no data regarding the use of allopurinol to overcome thiopurine-induced pancreatitis. Thus, if an adverse event occurs on AZA, it is worthwhile to have a trial of 6MP (initially at low dose) and, if that
fails, then the addition of low-dose allopurinol with 6MP, but only if a recurrence of the adverse event would be tolerated by the patient. If the adverse event occurs on 6MP
as the initial drug, anecdotal experience suggests a trial of AZA may also be worthwhile, followed by combination therapy if unsuccessful. Thiopurines have been the mainstay Proteasome inhibitor of treatment in IBD for many years and have also been extensively used in various rheumatological conditions. With the ability to measure thiopurine metabolites, important strides have been made in the IBD world to improve efficacy and optimize dosing of thiopurines, including in combination with low-dose allopurinol. In IBD, a therapeutic window of 230–260 to 450 pmol/10 × 88 RBCs has been established. Above this level, there are significantly
increased risks of side effects, including myelotoxicity, without any gain in efficacy. BCKDHB Studies in IBD have shown that over 30% of patients who would previously have been declared ‘refractory’ or ‘intolerant’ to thiopurines are now otherwise able to remain on monotherapy with improved clinical outcomes. Much of this work has yet to be undertaken within the rheumatology community. While the upper limit of 6TGN is a relevant threshold to apply in rheumatology due to the risk of universal side effects, the minimum effective 6TGN level is yet to be determined in different rheumatological conditions. The addition of allopurinol should also improve thiopurine metabolic profiles in rheumatology patients who are thiopurine shunters. It may be prudent for a rheumatology patient failing thiopurines to have their metabolites checked prior to drug cessation. “
“Hydrogen sulfide (H2S) is a gaseous mediator produced in the body. In experimental models, endogenously produced H2S has been shown to have pro-inflammatory effects. The aim of this study was to investigate whether H2S is present in three common rheumatic diseases, rheumatoid arthritis (RA), gout and osteoarthritis (OA) and to determine if H2S levels correlate with disease activity. Patients with RA, gout, OA, and healthy controls (n = 30 each) were recruited. Plasma and where possible, synovial fluid (SF), were obtained.